CXCR5 + CD8 + T Cell-mediated Suppression of Humoral Alloimmunity and AMR in Mice Is Optimized With MTOR and Impaired With Calcineurin Inhibition

Overview

Journal Transplantation

Specialty General Surgery

Date 2023 Oct 24

PMID 37872660

Authors

Jing L Han

Jason M Zimmerer

Qiang Zeng

Sachi R Chaudhari

Madison Hart

Anjali A Satoskar

Mahmoud Abdel-Rasoul

Christopher K Breuer

Ginny L Bumgardner

Affiliations

Soon will be listed here.

Abstract

Background: Adoptive cellular therapy (ACT) with antibody-suppressor CXCR5 + CD8 + T cells (CD8 + T Ab-supp ) inhibits alloantibody production, antibody-mediated rejection (AMR), and prolongs graft survival in multiple transplant mouse models. However, it is not known how conventional immunosuppressive agents impact the efficacy of CD8 + T Ab-supp ACT.

Methods: We investigated the efficacy of CD8 + T Ab-supp cell ACT when combined with calcineurin inhibitor (CNi) or mammalian target of rapamycin inhibitor (mTORi) in a murine model of kidney transplant.

Results: ACT-mediated decrease in germinal center B cells, posttransplant alloantibody titer, and amelioration of AMR in high alloantibody-producing CCR5 knockout kidney transplant recipients were impaired when ACT was combined with CNi and enhanced when combined with mTORi. CNi (but not mTORi) reduced ACT-mediated in vivo cytotoxicity of IgG + B cells and was associated with increased quantity of germinal center B cells. Neither CNi nor mTORi treatment impacted the expression of cytotoxic effector molecules (FasL, Lamp1, perforin, granzyme B) by CD8 + T Ab-supp after ACT. Concurrent treatment with CNi (but not mTORi) reduced in vivo proliferation of CD8 + T Ab-supp after ACT. The increase in quantity of splenic CD44 + CXCR5 + CD8 + T cells that occurs after ACT was reduced by concurrent treatment with CNi but not by concurrent treatment with mTORi (dose-dependent).

Conclusions: Impaired efficacy of ACT by CNi is attributed to reduced persistence and/or expansion of CD8 + T Ab-supp cells after ACT. In contrast, concurrent immunosuppression with mTORi preserves CD8 + T Ab-supp cells quantity, in vivo proliferation, and in vivo cytotoxic effector function after ACT and enhances suppression of humoral alloimmunity and AMR.

Citing Articles

Germinal Center B Cells are Uniquely Targeted by Antibody-Suppressor CXCR5CD8 T Cells.

Zimmerer J, Chaudhari S, Koneru K, Han J, Abdel-Rasoul M, Uwase H Transplant Direct. 2025; 11(2):e1742.

PMID: 39802197 PMC: 11723704. DOI: 10.1097/TXD.0000000000001742.

Antibody-Suppressor CXCR5+CD8+ T Cells Are More Potent Regulators of Humoral Alloimmunity after Kidney Transplant in Mice Compared to CD4+ Regulatory T Cells.

Han J, Zimmerer J, Zeng Q, Chaudhari S, Satoskar A, Abdel-Rasoul M J Immunol. 2024; 212(9):1504-1518.

PMID: 38517294 PMC: 11047759. DOI: 10.4049/jimmunol.2300289.

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